Útdráttur
Previous studies have indicated that conventional description of drug/cyclodextrin complexes in aqueous solutions as inclusion complexes are not as unambiguous as one might think. It has been shown that in some cases drug/cyclodextrin complexes consist of a mixture of inclusion and non-inclusion complexes. Furthermore it has been shown that drug/cyclodextrin complexes can form aggregates containing up to couple of hundred complexes. In this present study β-cyclodextrin (βCD) solubilization of hydrocortisone is enhanced by including short-chain anionic and cationic species in the aqueous complexation medium. For example, maximum hydrocortisone solubility in pure aqueous βCD solutions or suspensions is 2.2mg/ml. Addition of 1% (w/v) sodium acetate to the complexation medium increases this value to 7.1mg/ml (or over 220%). Further addition of 0.25% (w/v) hydroxypropyl methylcellulose to the medium increased the hydrocortisone solubility to over 9mg/ml. Similar results were obtained when sodium salicylate or benzalkonium chloride were added to the complexation medium. It is also shown that cyclodextrin complexes of lipophilic compounds that have good affinity for the cyclodextrin cavity can be used to enhance cyclodextrin solubilization of drugs that have low affinity for the cavity. All these observations can be explained by formation of drug/cyclodextrin complex aggregates.
| Upprunalegt tungumál | Enska |
|---|---|
| Síður (frá-til) | 101-107 |
| Síðufjöldi | 7 |
| Fræðitímarit | International Journal of Pharmaceutics |
| Bindi | 262 |
| Númer tölublaðs | 1-2 |
| DOI | |
| Útgáfustaða | Útgefið - 27 ágú. 2003 |
Athugasemd
Funding Information: Financial support for this investigation from the University of Iceland Research Fund is gratefully acknowledged. The skillful assistance of Ína B. Össurardóttir is gratefully appreciated.Fingerprint
Sökktu þér í rannsóknarefni „The effects of organic salts on the cyclodextrin solubilization of drugs“. Saman myndar þetta einstakt fingrafar.Vitna í þetta
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